干扰素- γ和白细胞介素-2增强细胞介导的抗同基因小鼠乳腺腺癌的细胞毒性。

Molecular biotherapy Pub Date : 1992-03-01
I Nakajima, T M Chu
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引用次数: 0

摘要

在体外和体内研究了小鼠重组干扰素- γ (ifn - γ)对细胞介导的肿瘤细胞毒性的影响,以自发性、弱免疫原性、同基因的小鼠乳腺腺癌(简称JC)为靶点。与ifn - γ预孵育的JC肿瘤细胞增加了细胞毒性T淋巴细胞和白细胞介素-2 (IL-2)诱导的淋巴因子激活杀伤细胞的裂解敏感性,并以ifn - γ剂量依赖的方式增加。与对照组相比,BALB/c小鼠背部JC肿瘤结节直接注射ifn - γ(10万U/d),连续5天,可降低肿瘤生长。同时腹腔注射IL-2 (300,000 IU/d),连续5天,这种抗肿瘤活性进一步增强。注射ifn - γ + IL-1后,肿瘤浸润淋巴细胞的表型检查显示,表达asialo GM1, L3T4和IL-2受体的细胞百分比增加。此外,在JC肿瘤细胞上检测到主要组织相容性复合体I类分子的表达增强。这些结果表明,在肿瘤内直接注射ifn - γ并同时给药IL-2,通过增强宿主细胞介导的免疫和靶细胞上主要组织相容性复合体I类抗原的表达,将具有潜在的临床价值。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Enhanced cell-mediated cytotoxicity by interferon-gamma and interleukin-2 against syngeneic murine mammary adenocarcinoma.

The effect of murine recombinant interferon-gamma (IFN-gamma) on cell-mediated cytotoxicity against tumor cells in vitro and in vivo was investigated using a spontaneously developed, weakly immunogenic, syngeneic murine mammary adenocarcinoma, designated JC, as the target. Preincubation of JC tumor cells with IFN-gamma increased the susceptibility of lysis by both cytotoxic T lymphocytes and interleukin-2 (IL-2)-induced lymphokine-activated killer cells in an IFN-gamma dose-dependent manner. A direct injection of IFN-gamma (10,0000 U/d) daily for 5 consecutive days into the JC tumor nodule on the backs of BALB/c mice reduced the tumor growth in comparison with that of the control group. This antitumor activity was further enhanced by combination with a simultaneous intraperitoneal injection of IL-2 (300,000 IU/d) daily for 5 consecutive days. Phenotypic examination of tumor-infiltrating lymphocytes after injection of IFN-gamma plus IL-1 revealed an increased percentage of the cells expressing asialo GM1, L3T4, and IL-2 receptors. Additionally, an enhanced expression of major histocompatibility complex class I molecules on the JC tumor cells was detected. These results indicated that a direct injection of IFN-gamma into the tumor accompanied with the administration of IL-2, by enhancing cell-mediated immunity of the hosts and expression of major histocompatibility complex class I antigens on target cells, will be of potential clinical value.

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